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高甘油三酯血症和多分散低密度脂蛋白受试者中载脂蛋白B的代谢

The metabolism of apolipoprotein B in subjects with hypertriglyceridemia and polydisperse LDL.

作者信息

Fisher W R, Zech L A, Bardalaye P, Warmke G, Berman M

出版信息

J Lipid Res. 1980 Aug;21(6):760-74.

PMID:7419987
Abstract

This research concerns the metabolism of apolipoprotein B (apoB) in hypertriglyceridemic subjects with polydisperse or heterogeneous LDL. Five subjects maintained under constant dietary control had blood samples fractionated into very low density lipoprotein (VLDL), Sf 20, Sf 10, and Sf 4 LDL, and plasma free leucine, and in three subjects VLDL was further fractionated by size. Apo B was isolated, and the masses of the plasma apo B pools were measured for these lipoproteins. Following injection of [3H]leucine as a metabolic tracer the specific activity of apo B in these lipoproteins and of plasma leucine were measured over 7 or 14 days. The kinetic data were examined using multicompartmental analysis and interpreted in terms of our previous model of apo B metabolism (1975. Federation Proc. 24: 2263.). Newly synthesized apo B, secreted as large VLDL, is metabolized by a delipidation chain yielding intermediate density lipoprotein (IDL), consisting of small VLDL and Sf 20 LDL, and eventually forms small, Sf4 LDL. LDL is metabolized in a steplike process from Sf 20 to Sf 10 and Sf 4 LDL. A second major biosynthetic input in apo B enters directly into IDL and 1/4 to 2/3 of newly synthesized apo B enters plasma by this route. Total apo B synthesis in these subjects is 5- to 10-fold greater than reported for normals. The rate of transport of VLDL apo B and IDL is slower than normal with a residence time which is increased about twofold; however, the VLDL apo B pool is enlarged 5- to 10-fold, and thus the quantity of apo B entering and leaving this pool per hour is much greater than in the normal. Two major pathways for apo B catabolism occur. Between 1/3 and 2/3 of apo B is metabolized through LDL, disappearing from plasma as Sf 4 LDL. The remainder of apo B disappears from plasma IDL directly. The four major findings in this kinetic study of apo B metabolism in hypertriglyceridemic subjects with polydisperse LDL are: 1) The marking increase in apo B synthesis; 2) the biosynthetic input of much of this apo B directly into IDL; 3) the large catabolic pathway of apo B which leaves IDL, and 4) the stepwise metabolism of LDL by which Sf 20, Sf 10 and Sf 4 LDL are generated.

摘要

本研究关注多分散或异质性低密度脂蛋白(LDL)的高甘油三酯血症患者载脂蛋白B(apoB)的代谢情况。5名维持恒定饮食控制的受试者的血样被分离为极低密度脂蛋白(VLDL)、Sf 20、Sf 10和Sf 4低密度脂蛋白,以及血浆游离亮氨酸,并且在3名受试者中,VLDL进一步按大小分离。分离出apo B,并测定这些脂蛋白的血浆apo B池的质量。注射[³H]亮氨酸作为代谢示踪剂后,在7天或14天内测定这些脂蛋白中apo B以及血浆亮氨酸的比活性。使用多室分析检查动力学数据,并根据我们之前的apo B代谢模型(1975年。联邦会议录。24: 2263.)进行解释。新合成的apo B以大的VLDL形式分泌,通过脱脂链代谢产生中间密度脂蛋白(IDL),IDL由小的VLDL和Sf 20低密度脂蛋白组成,最终形成小的Sf4低密度脂蛋白。LDL通过从Sf 20到Sf 10再到Sf 4低密度脂蛋白的逐步过程进行代谢。apo B的第二个主要生物合成输入直接进入IDL,并且新合成的apo B中有1/4到2/3通过此途径进入血浆。这些受试者中apo B的总合成量比正常人报道的高5至10倍。VLDL apo B和IDL的转运速率比正常慢,停留时间增加约两倍;然而,VLDL apo B池扩大了5至10倍,因此每小时进出该池的apo B量比正常人多得多。apo B分解代谢有两条主要途径。1/3至2/3的apo B通过LDL代谢,以Sf 4低密度脂蛋白的形式从血浆中消失。其余的apo B直接从血浆IDL中消失。在这项对具有多分散LDL的高甘油三酯血症患者apo B代谢的动力学研究中的四个主要发现是:1)apo B合成显著增加;2)大部分这种apo B直接生物合成输入到IDL中;3)apo B离开IDL的大分解代谢途径;4)LDL的逐步代谢,由此产生Sf 20、Sf 10和Sf 4低密度脂蛋白。

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